Cesano A, Visonneau S, Wolfe J H, Jeglum K A, Fernandez J, Gillio A, O'Reilly R J, Santoli D
Wistar Institute, Philadelphia, PA 19104, USA.
Cancer Immunol Immunother. 1997 May;44(3):125-36. doi: 10.1007/s002620050365.
The human MHC-non-restricted cytotoxic T cell line TALL-104 has been shown to display potent antitumor effects in several animal models with spontaneous and induced malignancies. In view of its potential future use in cancer therapy, we investigated the tolerability and target-organ toxicity of these cells in various animal species. The acute toxicity of TALL-104 cell administrations was evaluated in: (a) healthy immunocompetent mice and immunodeficient (SCID) mice bearing human tumors using multiple (up to 15) intraperitoneal (i.p.) injections, and (b) healthy dogs, tumor-bearing dogs, and healthy monkeys using multiple (up to 17) intravenous (i.v.) injections. TALL-104 cells were gamma-irradiated (40 Gy) prior to administration to mice and dogs, but administered without irradiation in monkeys. Cell doses ranged from 5 x 10(7)/kg to 10(10)/kg for each injection. All regimens were well tolerated, the main clinical signs observed being transient gastrointestinal effects. Moderate and transient increases in liver transaminase levels were observed in all animal species. Discrete and transient leukocytosis with neutrophilia was also noted in dogs and monkeys after i.v. injections of TALL-104 cells. Histological analysis revealed foci of hepatic necrosis with lympho-/mono-/granulocytic infiltration in immunocompetent mice injected i.p. with 5 x 10(9)-10(10) cells/kg. In the same mice, the colon showed an increased number of muciparous cells and alterations in the villi structure: these alterations were completely reversed by 72 h after the last injection, while liver alterations reversed more slowly (1 week). No delayed or chronic toxicity was observed in any of the animals even when non-irradiated TALL-104 cells were administered: both immunocompetent mice and healthy dogs were found to be grossly and histopathologically normal when sacrificed (1 year and 1 month after the last TALL-104 injection respectively). TALL-104 cells did not persist in these hosts. In addition, monkeys showed no molecular signs of TALL-104-cell-induced leukemia in their blood 1 year after the last cell injection. Despite immunosuppression, most of the tumor-bearing dogs as well as the healthy dogs and monkeys developed both humoral and cellular immune responses against TALL-104 cells. The data derived from these preclinical studies suggest that administration of high doses of irradiated TALL-104 cells is well tolerated and would be unlikely to induce severe toxicity if applied in clinical trials to the treatment of patients with refractory cancer.
人MHC非限制性细胞毒性T细胞系TALL-104已被证明在多种自发和诱发恶性肿瘤的动物模型中显示出强大的抗肿瘤作用。鉴于其未来在癌症治疗中的潜在用途,我们研究了这些细胞在各种动物物种中的耐受性和靶器官毒性。通过以下方式评估TALL-104细胞给药的急性毒性:(a) 使用多次(最多15次)腹腔内注射,对健康的免疫活性小鼠和携带人肿瘤的免疫缺陷(SCID)小鼠进行评估;(b) 使用多次(最多17次)静脉内注射,对健康犬、荷瘤犬和健康猴进行评估。在给小鼠和犬给药前,TALL-104细胞进行了γ射线照射(40 Gy),但给猴给药时未进行照射。每次注射的细胞剂量范围为5×10⁷/kg至10¹⁰/kg。所有给药方案耐受性良好,观察到的主要临床症状为短暂的胃肠道反应。在所有动物物种中均观察到肝转氨酶水平有中度和短暂升高。静脉注射TALL-104细胞后,犬和猴也出现了离散且短暂的白细胞增多伴中性粒细胞增多。组织学分析显示,腹腔注射5×10⁹ - 10¹⁰细胞/kg的免疫活性小鼠肝脏出现坏死灶,并伴有淋巴细胞/单核细胞/粒细胞浸润。在同一批小鼠中,结肠黏液分泌细胞数量增加,绒毛结构发生改变:这些改变在最后一次注射后72小时完全恢复,而肝脏改变恢复较慢(1周)。即使给予未照射的TALL-104细胞,在任何动物中均未观察到迟发性或慢性毒性:处死时(分别在最后一次注射TALL-104细胞后1年和1个月),免疫活性小鼠和健康犬的大体和组织病理学检查均正常。TALL-104细胞在这些宿主体内未持续存在。此外,在最后一次注射细胞1年后,猴的血液中未出现TALL-104细胞诱导白血病的分子迹象。尽管存在免疫抑制,大多数荷瘤犬以及健康犬和猴都产生了针对TALL-104细胞的体液免疫和细胞免疫反应。这些临床前研究的数据表明,给予高剂量的照射后TALL-104细胞耐受性良好,如果在临床试验中用于治疗难治性癌症患者,不太可能诱发严重毒性。
